Stereoselective Pharmacokinetics of Bisoprolol After Intravenous and Oral Administration in Beagle Dogs

Horikiri, Yuji; Suzuki, Takehiko; Mizobe, Masakazu

doi:10.1021/js960453v

Cited by 18 publications

(11 citation statements)

References 24 publications

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“…Differences in values have been reported in man for the unbound enantiomers of pindolol (Hsyu & Giacomini 1985;Somogyi et al 1992), disopyramide (Lima et al 1985) and amphetamine (Hutchaleelaha et al 1994); all underwent secretion in addition to filtration and, presumably, the observations reflected differences in secretory transport between isomers. However, there were no differences in the renal clearance of the unbound enantiomers of methadone (Foster et al 2000) and bisoprolol (Horikiri et al 1997), nor in inhibition by the enantiomers of pindolol, disopyramide and bupivacaine on the transport of tetraethylammonium across vesicles prepared from the apical membrane (referred to as brush-border membrane vesicles by the authors) (Gross & Somogyi 1994). Furthermore, inhibition by pindolol of the uptake of N-methylnicotinamide by these vesicles was not stereoselective (Ott et al 1991).…”

Section: Discussionmentioning

confidence: 99%

Effect of ketoprofen and its enantiomers on the renal disposition of methotrexate in the isolated perfused rat kidney

Karpf

Kirkegaard

Evans

et al. 2003

Journal of Pharmacy and Pharmacology

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Non-steroidal anti-inflammatory drugs (NSAIDs) have been shown to inhibit the renal tubular secretion of methotrexate. However, the relative contribution of the active S- and inactive R-enantiomers is unknown. This study examined the effect of racemic ketoprofen and its enantiomers on the renal disposition of methotrexate in the isolated perfused rat kidney (IPK). Nineteen kidneys were divided between a control and three treatment groups. Controls were perfused with methotrexate alone (25 micrograms mL-1, n = 5) over three 30-min periods. Treatment groups were perfused with methotrexate (25 micrograms m-1) for the first period, followed by a second period of methotrexate (25 micrograms mL-1) plus R- (n = 5), S- (n = 5) or RS-ketoprofen (n = 4) at 25 micrograms mL-1, and a third period of methotrexate (25 micrograms mL-1) plus R-, S- or RS-ketoprofen (50 micrograms mL-1). Perfusate and urine were collected over 10-min intervals. Methotrexate was measured by HPLC and its binding in perfusate by ultrafiltration. The clearance ratio (CR) for methotrexate was obtained by dividing the renal clearance by the product of its fraction unbound and the glomerular filtration rate. During control experiments, there was no significant change in the CR over 90 min. R-, S- and RS-ketoprofen at 50 micrograms mL-1 reduced the CR of methotrexate significantly, but there was no difference between the three groups. While the enantiomers of ketoprofen reduced the renal excretion of methotrexate, the interaction was not enantioselective.

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Section: Discussionmentioning

confidence: 99%

Effect of ketoprofen and its enantiomers on the renal disposition of methotrexate in the isolated perfused rat kidney

Karpf

Kirkegaard

Evans

et al. 2003

Journal of Pharmacy and Pharmacology

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“…In the previous study, 10 the distinctive stereoselectivity in the pharmacokinetics of bisoprolol in dogs was found when racemic bisoprolol was intravenously and orally administered. The plasma AUC and half-life of (S)-(-)bisoprolol were significantly greater than those of (R)-(+)bisoprolol.…”

Section: Introductionmentioning

confidence: 91%

“…Therefore, it was concluded that the stereoselective disposition of enantiomers in dogs was brought about by a difference in the metabolic clearance between (S)-(-)-and (R)-(+)-bisoprolol. 10 The aim of the present study was to characterize the difference in plasma and urinary pharmacokinetics of bisoprolol enantiomers in human subjects. In addition, an in vitro study was performed to assess the role of human cytochrome P450 (CYP) isoforms in mediating the major pathways of bisoprolol metabolism.…”

Section: Introductionmentioning

confidence: 99%

Pharmacokinetics and Metabolism of Bisoprolol Enantiomers in Humans

Horikiri

Suzuki

Mizobe

1998

Journal of Pharmaceutical Sciences

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The plasma concentrations and urinary excretions of bisoprolol enantiomers in four Japanese male healthy volunteers after a single oral administration of 20 mg of racemic bisoprolol were evaluated. The AUC(infinity) and elimination half-life of (S)-(-)-bisoprolol were slightly larger than those of (R)-(+)-bisoprolol in all subjects. The metabolic clearance of (R)-(+)-bisoprolol was significantly (P < 0.05) larger than that of (S)-(-)-bisoprolol (S/R ratio: 0.79+/-0.03), although the difference was small. In contrast, no stereoselective in vitro protein binding of bisoprolol in human plasma was found. An in vitro metabolic study using recombinant human cytochrome P450 (CYP) isoforms indicated that oxidation of both bisoprolol enantiomers was catalyzed by the two isoforms, CYP2D6 and CYP3A4. CYP2D6 metabolized bisoprolol stereoselectively (R > S), whereas the metabolism of bisoprolol by CYP3A4 was not stereoselective. The S/R ratio of the mean clearance due to renal tubular secretion was 0.68, indicating a moderate degree of stereoselective renal tubular secretion. These findings taken together suggest that the small differences in the pharmacokinetics between (S)-(-)- and (R)-(+)-bisoprolol are mainly due to the stereoselectivity in the intrinsic metabolic clearance by CYP2D6 and renal tubular secretion.

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“…To appropriately define the process mechanistically, blood measurements and clearance by that pathway should be determined. A good example of this is provided by bisoprolol [73]. The urinary recovery ratio of S:R enantiomer was 1.29 in urine, whereas renal clearance was essentially nonstereoselective (S:R ratio ¼ 0:96).…”

Section: Excretionmentioning

confidence: 99%

Drug disposition in three dimensions: an update on stereoselectivity in pharmacokinetics

Brocks

2006

Biopharm. Drug Dispos.

134

108

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Many marketed drugs are chiral and are administered as the racemate, a 50:50 combination of two enantiomers. Pharmacodynamic and pharmacokinetic differences between enantiomers are well documented. Because of enantioselectivity in pharmacokinetics, results of in vitro pharmacodynamic studies involving enantiomers may differ from those in vivo where pharmacokinetic processes will proceed. With respect to pharmacokinetics, disparate plasma concentration vs time curves of enantiomers may result from the pharmacokinetic processes proceeding at different rates for the two enantiomers. At their foundation, pharmacokinetic processes may be enantioselective at the levels of drug absorption, distribution, metabolism and excretion. In some circumstances, one enantiomer can be chemically or biochemically inverted to its antipode in a unidirectional or bidirectional manner. Genetic consideration such as polymorphic drug metabolism and gender, and patient factors such as age, disease state and concomitant drug intake can all play a role in determining the relative plasma concentrations of the enantiomers of a racemic drug. The use of a nonstereoselective assay method for a racemic compound can lead to difficulties in interpretation of data from, for example, bioequivalence or dose/concentration vs effect assessments. In this review data from a number of representative studies involving pharmacokinetics of chiral drugs are presented and discussed.

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Stereoselective Pharmacokinetics of Bisoprolol After Intravenous and Oral Administration in Beagle Dogs

Cited by 18 publications

References 24 publications

Effect of ketoprofen and its enantiomers on the renal disposition of methotrexate in the isolated perfused rat kidney

Effect of ketoprofen and its enantiomers on the renal disposition of methotrexate in the isolated perfused rat kidney

Pharmacokinetics and Metabolism of Bisoprolol Enantiomers in Humans

Drug disposition in three dimensions: an update on stereoselectivity in pharmacokinetics

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